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核凝聚与自由基清除:双苯并咪唑调节辐射对DNA损伤的双重机制。

Nuclear condensation and free radical scavenging: a dual mechanism of bisbenzimidazoles to modulate radiation damage to DNA.

作者信息

Tawar Urmila, Bansal Sandhya, Shrimal Shiteshu, Singh Manish, Tandon Vibha

机构信息

Dr. B. R. Ambedkar Center for Biomedical Research, University of Delhi, Delhi, 110007, India.

出版信息

Mol Cell Biochem. 2007 Nov;305(1-2):221-33. doi: 10.1007/s11010-007-9546-y. Epub 2007 Jul 10.

Abstract

The complexing of histones with DNA and the resulting condensation of chromatin protects mammalian cell, from radiation-induced strand breakage. In the present study, benzimidazoles DMA and TBZ showed marked radioprotection through drug-induced compaction of chromatin and direct quenching of free radicals generated by radiation. The mammalian cells were incubated with 100 microM concentration of DMA and TBZ and irradiated at 5 Gy; both the ligands showed nuclei condensation suggesting a probable mechanism to protect DNA from radiation damage. The bisubstituted analogs of Hoechst 33342 are found to be better free radical scavengers and protect DNA against radiation-induced damage at a lower concentration than the parent molecule. Both the ligands also quenched free radicals in isolated free radical system suggesting their dual mode of action against radiation-induced damage to DNA. Molecules binding to the chromatin alter gene expression, whereas in this study both the ligands have not shown any profound effect on the nucleosome assembly and gene expression in vitro and in vivo. Both ligands afford a 2-fold protection by altering DNA structure as well as through direct free radical quenching in bulk solution in comparison to the parent ligand, which acts only through quenching of free radicals.

摘要

组蛋白与DNA的络合以及由此产生的染色质凝聚可保护哺乳动物细胞免受辐射诱导的链断裂。在本研究中,苯并咪唑DMA和TBZ通过药物诱导的染色质压缩和对辐射产生的自由基的直接淬灭表现出显著的辐射防护作用。将哺乳动物细胞与100微摩尔浓度的DMA和TBZ孵育,并以5 Gy进行辐照;两种配体均显示出细胞核凝聚,提示了一种保护DNA免受辐射损伤的可能机制。发现Hoechst 33342的双取代类似物是更好的自由基清除剂,并且在比母体分子更低的浓度下就能保护DNA免受辐射诱导的损伤。两种配体在分离的自由基体系中也能淬灭自由基,表明它们对辐射诱导的DNA损伤具有双重作用模式。与染色质结合的分子会改变基因表达,而在本研究中,两种配体在体外和体内均未对核小体组装和基因表达表现出任何显著影响。与仅通过淬灭自由基起作用的母体配体相比,两种配体通过改变DNA结构以及在本体溶液中直接淬灭自由基,提供了2倍的保护作用。

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